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Trophic effects of androgen: development and hormonal regulation of neuron number in a sexually dimorphic vocal motor nucleus.

机译:雄激素的营养作用:性双态声带运动神经核中神经元数量的发育和激素调节。

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In Xenopus laevis, the laryngeal motor nucleus (n. of cranial nerves IX-X) is part of a sexually differentiated, androgen sensitive neuromuscular system devoted to vocalization. Adult males have more n. IX-X neurons than females; however, during development of n. IX-X, the rate of neurogenesis does not appear to differ between the sexes. In this study, we explored the role of naturally occurring cell death in the development of this nucleus and asked whether cell death might be involved in establishing the sex difference in neuron number. Counts of n. IX-X neurons reveal that at tadpole stage 56, males and females have similar numbers of n. IX-X neurons, but by stage 64 male neuron numbers are greater. This sex difference arises owing to a greater net loss of neurons in females-males lose approximately 25% of their n. IX-X neurons between stages 56 and 64, while females lose approximately 47%. Sexual differentiation of n. IX-X neuron number coincides with a period of developmental cell death, as evidenced by terminal transferase-mediated dUTP nick-end labeling and the presence of pyknotic nuclei in n. IX-X. A role for gonadal hormones in controlling cell number was examined by treating tadpoles with exogenous androgen and determining the number of n. IX-X neurons at stage 64. Dihydrotestosterone (DHT) treatment from the beginning of the cell death period (stage 54) until stage 64 had no effect on the number of n. IX-X neurons in males but did significantly increase n. IX-X neuron number in females. This increase was sufficient to abolish the sex difference normally observed at stage 64. Although DHT induced increases in female neuron number, it did not induce increases in cell proliferation or addition of newly born neurons to n. IX-X. DHT may therefore have increased neuron number by protecting cells from death. We conclude that androgens can influence the survival of n. IX-X neurons during a period of naturally occurring cell death, and that this action of androgen is critical to the development of sex differences in n. IX-X neuron number. Copyright 1999 John Wiley & Sons, Inc.
机译:在非洲爪蟾中,喉运动核(颅神经IX-X)是性分化的雄激素敏感神经肌肉系统的一部分,专门用于发声。成年男性更多。 IX-X神经元多于雌性;但是,在n的开发过程中。 IX-X,两性之间的神经发生率似乎没有差异。在这项研究中,我们探索了自然发生的细胞死亡在该核发育中的作用,并询问细胞死亡是否可能与建立神经元数量的性别差异有关。计数n。 IX-X神经元显示,在t期56岁,雄性和雌性的n数量相似。 IX-X神经元,但是到了阶段64男性神经元的数量更大。这种性别差异的产生是由于雌性神经元的净损失更大,而雄性则损失了其n的25%。在第56到64阶段之间的IX-X神经元,而雌性则损失约47%。 n的性别分化IX-X神经元数目与发育细胞死亡的时期相吻合,这可以通过末端转移酶介导的dUTP缺口末端标记和n中存在缩酮核来证明。 IX-X。通过用外源雄激素处理t并确定n的数量,研究了性腺激素在控制细胞数量中的作用。第64阶段的IX-X神经元。从细胞死亡期开始(第54阶段)到第64阶段的二氢睾酮(DHT)处理对n的数量没有影响。男性的IX-X神经元,但确实显着增加n。女性的IX-X神经元数。这种增加足以消除通常在第64阶段观察到的性别差异。尽管DHT诱导了雌性神经元数量的增加,但它并未诱导细胞增殖的增加或n中新生神经元的增加。 IX-X。因此,DHT可能通过保护细胞免于死亡而增加了神经元数量。我们得出结论,雄激素可以影响n的存活。 IX-X神经元在自然发生的细胞死亡期间,并且雄激素的这种作用对于n中性别差异的发展至关重要。 IX-X神经元编号。版权所有1999 John Wiley&Sons,Inc.

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